Djurendić Evgenija, Daljev Jovana, Sakac Marija, Canadi Janos, Santa Suzana Jovanović, Andrić Silvana, Klisurić Olivera, Kojić Vesna, Bogdanović Gordana, Djurendić-Brenesel Maja, Novaković Sladjana, Gasi Katarina Penov
Department of Chemistry, Faculty of Sciences, University of Novi Sad, Trg Dositeja Obradovića 3, 21 000 Novi Sad, Serbia.
Steroids. 2008 Jan;73(1):129-38. doi: 10.1016/j.steroids.2007.09.005. Epub 2007 Sep 22.
Steroidal epoxy and/or N-oxy 17-picolyl and 17-picolinylidene-androst-5-ene derivatives have been prepared using 3beta,17beta-dihydroxy-17alpha-picolyl-androst-5-ene (1), 3beta-acetoxy-17-picolinylidene-androst-5-ene (2), and 3beta-hydroxy-17-picolinylidene-androst-5-ene (3) as synthetic precursors. The compounds 2 and/or 3 were reacted with m-chloroperoxybenzoic acid (MCPBA). The compounds synthesized from 2 were 17-picolinylidene-N-oxide 4, 5alpha,6alpha-epoxy and 5beta,6beta-epoxy-17-picolinylidene-N-oxide 5 and 6, and 5alpha,6alpha:17alpha,20alpha- and 5beta,6beta:17alpha,20alpha-diepoxy-N-oxide 7 and 8. Starting from compound 3, a mixture of 5alpha,6alpha-epoxy and 5beta,6beta-epoxy-17-picolinylidene 9 and 10, 5alpha,6alpha-epoxy and 5beta,6beta-epoxy-17-picolinylidene-N-oxide 11 and 12, and 5alpha,6alpha:17alpha,20alpha- and 5beta,6beta:17alpha,20alpha-diepoxy-N-oxide 13 and 14 were obtained. From compounds 15 and 18, obtained from 1 and 3 by the Oppenauer oxidation, the 4alpha,5alpha-epoxy and 4beta,5beta-epoxy derivatives 16, 17 and 20, 21 were prepared by oxidation with 30% H(2)O(2). Oxidation of 18 with MCPBA yielded only the N-oxide 19. The structures of compounds 15 and 18 were proved by the X-ray analysis. Compounds 1-6, 9, 15, 17, 18, and 21 were tested on activity against the enzyme aromatase. Antitumor activity against three tumor cell lines (human breast adenocarcinoma ER+, MCF-7, human breast adenocarcinoma ER-, MDA-MB-231, and prostate cancer PC3) was evaluated. Three tested compounds (1, 4, and 19) showed strong activity against PC3, the IC(50) values being in the range 0.55-10microM, whereas compound 17 showed strong activity against MDA-MB-231 (IC(50) 10.4microM).
已使用3β,17β - 二羟基 - 17α - 吡啶甲基 - 雄甾 - 5 - 烯(1)、3β - 乙酰氧基 - 17 - 吡啶亚甲基 - 雄甾 - 5 - 烯(2)和3β - 羟基 - 17 - 吡啶亚甲基 - 雄甾 - 5 - 烯(3)作为合成前体来制备甾体环氧和/或N - 氧基17 - 吡啶甲基和17 - 吡啶亚甲基 - 雄甾 - 5 - 烯衍生物。化合物2和/或3与间氯过氧苯甲酸(MCPBA)反应。由2合成的化合物有17 - 吡啶亚甲基 - N - 氧化物4、5α,6α - 环氧和5β,6β - 环氧 - 17 - 吡啶亚甲基 - N - 氧化物5和6,以及5α,6α:17α,20α - 和5β,6β:17α,20α - 二环氧 - N - 氧化物7和8。从化合物3开始,得到了5α,6α - 环氧和5β,6β - 环氧 - 17 - 吡啶亚甲基9和10、5α,6α - 环氧和5β,6β - 环氧 - 17 - 吡啶亚甲基 - N - 氧化物11和12,以及5α,6α:17α,20α - 和5β,6β:17α,20α - 二环氧 - N - 氧化物13和14的混合物。通过欧芬脑尔氧化反应由1和3得到化合物15和18,再用30% H₂O₂氧化制备出4α,5α - 环氧和4β,5β - 环氧衍生物16、17和20、21。用MCPBA氧化18仅得到N - 氧化物19。化合物结构15和18经X射线分析得以证实。对化合物1 - 6、9、15、17、18和21进行了抗芳香化酶活性测试。评估了其对三种肿瘤细胞系(人乳腺腺癌ER + ,MCF - 7;人乳腺腺癌ER - ,MDA - MB - 231;前列腺癌PC3)的抗肿瘤活性。三种受试化合物(1、4和19)对PC3显示出强活性,IC₅₀值在0.55 - 10μM范围内,而化合物17对MDA - MB - 231显示出强活性(IC₅₀为10.4μM)。
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